Immunometabolism in Caenorhabditis elegans

metabolism is profoundly altered during bacterial infection, as a consequence of immune activation and secondary to virulence strategies of invading pathogens. As a the metabolic pathways regulate nutrient energy resource in to pathogen in order to meet the physiological of the during the specific alterations in host metabolism occur during bacterial infection are in organ systems that occur during and metabolic interactions between the and the nematode starting to characterize principles of of food and agents of C . elegans immune defenses coordinated by epithelial C to define changes in metabolism specifically by in the intestine. immune response and ability survive pathogen is heavily influenced by pathogen-induced changes in host


Insulin signaling integrates host metabolism, pathogen resistance, and longevity
The insulin/insulin-like growth factor signaling pathway integrates host nutritional status and environmental cues to control core physiological processes in C. elegans, including metabolism, growth rate, behavior, and stress resistance [1]. Activation of the C. elegans insulin/IGF-1 transmembrane receptor (IGFR) ortholog DAF-2 by insulin-like peptides results in the phosphorylation of the Foxo transcription factor DAF-16, causing it to be sequestered in the cytoplasm [2]. Low activity of DAF-2 allows DAF-16 to translocate to the nucleus where it controls the transcriptional output of this pathway [3]. Constitutive activation of DAF-16 in daf-2 lossof-function mutants extends nematode life span up to 3 times than that of wild-type animals and drives resistance to both abiotic stresses and pathogen infection [4,5]. In addition, de novo lipogenesis is increased in daf-2 mutants, which leads to accumulation of somatic fat. The pathogen resistance and life span extension phenotype of daf-2 mutants require the p38 mitogen-activated protein kinase (MAPK) PMK-1 pathway, a critical innate immune pathway in C. elegans [6]. However, the transcriptional targets of the DAF-2/DAF-16 and the p38 MAPK PMK-1 pathways during pathogen infection have essentially no overlap, suggesting that these pathways operate in parallel to promote resistance to pathogen infection [6]. Interestingly, infection by the bacterial pathogen Pseudomonas aeruginosa activates DAF-2 signaling as an offensive mechanism to suppress host immune defenses by causing DAF-16 to be sequestered in the cytoplasm [7]. Insulin/insulin-like growth factor signaling is strongly conserved across

Allocation of lipid resources affects physiological trade-offs between pathogen resistance, life span, and reproduction
Studies of immunometabolism in C. elegans have uncovered trade-offs between immune activation and lipid homeostasis that affect pathogen resistance, reproduction, and life span. The cytoprotective transcription factor SKN-1, the C. elegans ortholog of mammalian Nrf2, coordinates transcriptional responses that restore cellular homeostasis during oxidative, proteotoxic, and metabolic stresses and also provides protection during pathogen infection [8,9]. During bacterial infection, activation of SKN-1 promotes resistance to pathogen-derived toxins and drives redistribution of fat from the soma to the germline [10]. However, altered lipid homeostasis in C. elegans with unchecked SKN-1 activation has lasting deleterious effects, which impair organismal health later in life [10]. Thus, the activity of SKN-1 is closely regulated, in part through epigenetic modifications, which redirect its transcriptional output to meet the physiological need [10].
In addition, pathogen and stress-resistance programs are suppressed as animals increase resource investment to promote reproductive success. Two conserved homeodomain transcription factors CEH-60/PBX and UNC-62/MEIS function as a heterodimer to promote the synthesis of lipoproteins, which shuttle lipids to the germline to support embryogenesis. In addition, the CEH-60:UNC-62 complex also suppresses genes, which are important for pathogen defense and longevity [11]. Similarly, TCER-1, a transcription elongation and splicing factor, promotes reproductive fitness and lipid synthesis at the expense of pathogen and abiotic stress defenses [12]. Finally, a core host defense pathway in C. elegans, the p38 MAP PMK-1 pathway, is activated by nutrient signals independently of canonical mechanisms that sense food availability and accelerates aging when it is aberrantly induced, providing an example of the deleterious effects of immune activation on longevity [13].

Lipid metabolism is required for immune activation and pathogen defense
C. elegans pathogenesis assays have defined requirements for specific lipids and lipogenesis enzymes in innate immune regulation and pathogen defense. C. elegans can synthesize the full range of fatty acid molecules de novo and thus does not have a dietary requirement for specific fatty acids. Monounsaturated and polyunsaturated fatty acids are synthesized through sequential action of conserved elongase (elo) and desaturase (fat) genes. The Δ6-desaturase fat-3, which produces the polyunsaturated fatty acids gamma-linoleic acid and stearidonic acid, is required for the basal expression of innate immune genes and resistance to infection by the bacterial pathogen P. aeruginosa [14]. In addition, the 2 stearoyl-coenzyme A desaturases that synthesize the monounsaturated fatty acid oleate in C. elegans, fat-6 and fat-7, are required for the induction of innate immune genes [15]. Accordingly, nematodes with loss-of-function mutations in fat-6 and fat-7 are hypersusceptible to infection by diverse pathogens, which can be rescued by the addition of exogenous oleate [15].
Additionally, low levels of s-Adenosylmethionie (SAM), the methyl donor that modifies nucleic acids and histones and is involved in producing phospholipids, result in a decrease in phosphatidylcholine (PC). Low levels of PC in animals that lack sams-1, an enzyme that produces SAM, induce expression of lipogenesis genes resulting in lipid droplet accumulation [16,17]. Interestingly, low PC increases the basal expression of immune genes in C. elegans feeding on nonpathogenic food. However, low levels of activating histone methylation in these animals also limit pathogen-responsive transcription and renders animals more susceptible to infection [16].
Together, these studies in C. elegans reveal novel connections between nutrient stores, metabolism, and host susceptibility to bacterial infection.

Mitochondria link energy metabolism and immune activation
Mitochondria are required for multiple aspects of cellular metabolism. Bacteria often target mitochondria during infection as an offensive strategy to promote tissue damage. For example, P. aeruginosa secretes phenazine toxins, electron shuttles that disrupt mitochondrial function, [18] and Streptomyces sp. elaborate antimycin A and oligomycin, inhibitors of mitochondrial respiration that are widely used in the laboratory. Studies in C. elegans have characterized several host countermeasures that have evolved to detect mitochondrial dysfunction as a sign of pathogen infection.
The unfolded protein response in mitochondria (UPR mt ) is regulated by the transcription factor ATFS-1, a unique protein that contains both a nuclear localization (NLS) and a mitochondrial targeting sequence (MTS) [19,20]. Healthy mitochondria import ATFS-1 efficiently, but during mitochondrial dysfunction, protein import is impaired, and ATFS-1 accumulates in the cytoplasm, where it can traffic to the nucleus via its NLS. ATFS-1 activates a transcriptional program in the nucleus that promotes both recovery of mitochondrial function and defense against pathogen infection through the induction of secreted innate immune effectors [19,20]. Interestingly, the pathogen P. aeruginosa evolved mechanisms to suppress the UPR mt by exploiting a host pathway that negatively regulates ATFS-1 [18].
In addition, ceramides, a class of host lipids, protect C. elegans from mitochondrial dysfunction induced by toxins or pathogen exposure [21]. Likewise, disruption of mitochondrial function activates the nuclear hormone receptor nhr-45, which induces detoxification programs that provide protection during pathogen infection [22]. Finally, the iron-binding siderophore pyoverdine, which is produced by P. aeruginosa, causes mitochondrial dysfunction during infection, which engages protective destruction of damaged mitochondria (mitophagy) [23].
Together, these studies demonstrate that mitochondrial function is closely guarded by host surveillance pathways that function to restore homeostasis and activate protective innate immune defenses.

Transcriptional control of innate immunity and metabolism by conserved nuclear hormone receptors
The C. elegans genome encodes a large number of nuclear hormone receptors (NHRs), unique transcription factors that program adaptive transcriptional responses following recognition of specific ligands, such as fatty acids, metabolites, hormones, and xenobiotics. NHRs regulate a number of basic biological processes in C. elegans, including lipid and cholesterol metabolism, life span, development, and anti-pathogen defenses. The marked expansion of NHRs in nematodes-284 NHRs are present in C. elegans, whereas Drosophila and humans have only 21 and 48, respectively-suggests that these proteins may play particularly important roles in nematode physiology, such as the integration of host metabolism with innate immunity to promote resistance to pathogen infection.
Interestingly, 264 of the 284 NHRs in the C. elegans genome are orthologous to the alpha isoform of the mammalian nuclear receptor hepatocyte nuclear factor 4 (HNF4). HNF4 is expressed in the intestinal epithelium and in hepatocytes and has been implicated in the control of intestinal inflammation and the pathogenesis of inflammatory bowel disease and cancer. In C. elegans, the HNF4 homolog NHR-86 surveys the chemical environment to activate protective anti-pathogen defenses by binding to the promoters of immune effector genes [24]. These data suggest that the expansion of the HNF4 family in C. elegans may have been fueled, at least in part, by the roles of these proteins in the activation of host defense responses. In addition, the C. elegans homolog of peroxisome proliferator-activated receptor (PPAR), NHR-49, a central regulator of fat metabolism, is required for resistance to multiple gram-positive bacteria, including Enterococcus faecalis [25]. Of note, NHR-49 interacts with a conserved subunit of the Mediator complex MDT-15/MED15 to control the production of fatty acids, and a separate study found that MDT-15 also coordinates immune defenses during pathogen infection [26]. Thus, NHR-49 and MDT-15 regulation of fatty acid metabolism may support immune function in nematodes. In addition, the C. elegans homolog of the liver X receptor (LXR), NHR-8, which controls cholesterol and bile acid homeostasis, is required for defense against infection with P. aeruginosa [27,28]. Finally, the nuclear hormone receptor NHR-14 links iron availability with the induction of innate immune defenses that provide protection from pathogen infection [29].
In summary, NHRs are able to mount rapid transcriptional responses to specific intracellular and extracellular cues and are thus poised to integrate host physiology and metabolism to provide protection from pathogens during infection. Future studies of the mechanisms by which NHRs control immunometabolism in C. elegans are of particular interest.